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PigmentaryTSC markerICD-10 L81.6

Hypomelanotic macule (ash-leaf macule)

Ash-leaf macule; ash-leaf spot; hypopigmented macule of tuberous sclerosis; congenital hypomelanosis

Hypomelanotic macules are congenital or early-childhood hypopigmented patches that are present in approximately 90% of patients with tuberous sclerosis complex (TSC) and are usually the earliest detectable cutaneous sign. Classical lance-ovate ("ash-leaf") shape with a tapered end accounts for ~ 50% of TSC macules. ≥ 3 macules of ≥ 5 mm diameter is a major diagnostic criterion of TSC (2012 consensus, updated 2021). They are usually present at birth or appear in infancy; Wood's lamp examination accentuates the pale patches and is invaluable in pale-skinned infants where lesions may be subtle. Hypomelanotic macules are functionally and cosmetically benign but their identification is critical for TSC diagnosis and surveillance.

CurrentLast reviewed 15 May 2026

Clinical features

  • Hypopigmented (not depigmented) macule with poorly-demarcated borders — Wood's lamp emphasises the patch.
  • Common shapes:
    • Lance-ovate or "ash-leaf" — tapered at one or both ends (50%).
    • Polygonal / "thumbprint" (40%).
    • "Confetti" macules — multiple tiny hypopigmented dots, < 5 mm, on shins / forearms (~ 30% of TSC adults).
  • Sites — any but typically trunk, buttocks, lower limbs.
  • Present at birth or appear in infancy; persist lifelong.
  • White lock of hair (poliosis) — a hypomelanotic feature of the scalp.

Tuberous sclerosis complex

  • Hypomelanotic macules are one of the major diagnostic criteria of TSC (2021 International Consensus Conference):
    • Hypomelanotic macules — ≥ 3, at least 5 mm diameter — is a major criterion.
    • Confetti skin lesions are a minor criterion.
    • Other major skin features — facial angiofibromas (≥ 3), shagreen patch, ungual fibromas (≥ 2).
  • Definite TSC diagnosis — two major OR one major + two minor criteria OR pathogenic TSC1 / TSC2 germline variant.
  • Refer for TSC evaluation if ≥ 3 hypomelanotic macules of ≥ 5 mm are identified:
    • Family history, seizures, developmental delay, autism.
    • Skin examination — facial angiofibromas, shagreen patch, ungual fibromas.
    • Eye examination — retinal hamartomas.
    • Brain MRI — tubers, subependymal nodules, SEGA.
    • Cardiac echo — rhabdomyomas (infant); resolve over time.
    • Renal ultrasound — angiomyolipomas.
    • Lung CT in women — lymphangioleiomyomatosis (LAM).
    • Genetic testing — TSC1 / TSC2.
  • See tuberous sclerosis for management.

Differential — congenital hypopigmentation

  • Naevus depigmentosus — congenital, stable; segmental or focal; no syndromic association.
  • Piebaldism — bilateral, symmetric, anterior; white forelock; KIT mutation.
  • Vitiligo — acquired complete depigmentation; sharp border; autoimmune.
  • Hypomelanosis of Ito (incontinentia pigmenti achromians) — segmental hypopigmentation along Blaschko lines; neurological / musculoskeletal anomalies.
  • Post-inflammatory hypopigmentation — preceding eczema / trauma.
  • Pityriasis alba — atopic; ill-defined.

References

  1. Northrup H et al. Updated international tuberous sclerosis complex diagnostic criteria and surveillance and management recommendations. Pediatr Neurol; 2021.
  2. Krueger DA et al. Tuberous sclerosis complex — surveillance and management. Pediatr Neurol; 2013.

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